Do DNA Double-Strand Breaks Drive Aging?

Ryan R White; Jan Vijg

doi:10.1016/j.molcel.2016.08.004

Do DNA Double-Strand Breaks Drive Aging?

Mol Cell. 2016 Sep 1;63(5):729-38. doi: 10.1016/j.molcel.2016.08.004.

Authors

Ryan R White¹, Jan Vijg²

Affiliations

¹ Department of Genetics, Albert Einstein College of Medicine, 1301 Morris Park Ave., Bronx, NY 10461, USA. Electronic address: rwhite@rockefeller.edu.
² Department of Genetics, Albert Einstein College of Medicine, 1301 Morris Park Ave., Bronx, NY 10461, USA. Electronic address: jan.vijg@einstein.yu.edu.

Abstract

DNA double-strand breaks (DSBs) are rare, but highly toxic, lesions requiring orchestrated and conserved machinery to prevent adverse consequences, such as cell death and cancer-causing genome structural mutations. DSBs trigger the DNA damage response (DDR) that directs a cell to repair the break, undergo apoptosis, or become senescent. There is increasing evidence that the various endpoints of DSB processing by different cells and tissues are part of the aging phenotype, with each stage of the DDR associated with specific aging pathologies. In this Perspective, we discuss the possibility that DSBs are major drivers of intrinsic aging, highlighting the dynamics of spontaneous DSBs in relation to aging, the distinct age-related pathologies induced by DSBs, and the segmental progeroid phenotypes in humans and mice with genetic defects in DSB repair. A model is presented as to how DSBs could drive some of the basic mechanisms underlying age-related functional decline and death.

Publication types

Review

MeSH terms

Acid Anhydride Hydrolases
Aging / genetics*
Aging / metabolism
Aging / pathology
Animals
BRCA1 Protein / genetics
BRCA1 Protein / metabolism
Cell Cycle Proteins / genetics
Cell Cycle Proteins / metabolism
Cellular Senescence
DNA / genetics*
DNA / metabolism
DNA Breaks, Double-Stranded*
DNA Repair Enzymes / genetics
DNA Repair Enzymes / metabolism
DNA Repair*
DNA-Binding Proteins / genetics
DNA-Binding Proteins / metabolism
Endonucleases / genetics
Endonucleases / metabolism
Gene Expression Regulation*
Humans
Ku Autoantigen / genetics
Ku Autoantigen / metabolism
MRE11 Homologue Protein
Mice
Models, Genetic
Nuclear Proteins / genetics
Nuclear Proteins / metabolism
Progeria / genetics*
Progeria / metabolism
Progeria / pathology
Saccharomyces cerevisiae / genetics
Saccharomyces cerevisiae / metabolism
Signal Transduction

Substances

BRCA1 Protein
BRCA1 protein, human
Cell Cycle Proteins
DNA-Binding Proteins
MRE11 protein, human
NBN protein, human
Nuclear Proteins
DNA
ERCC1 protein, human
Endonucleases
MRE11 Homologue Protein
Acid Anhydride Hydrolases
RAD50 protein, human
Ku Autoantigen
DNA Repair Enzymes

Abstract

Publication types

MeSH terms

Substances

Grants and funding